ADHESION, GROWTH AND MORPHOLOGY OF HUMAN MESOTHELIAL CELLS ON
Normal histology Layers: -Mucosa -Submucosa -Muscularis propria (externa) -Subserosa Serosa -...
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Transcript of Normal histology Layers: -Mucosa -Submucosa -Muscularis propria (externa) -Subserosa Serosa -...
Normal histology
• Layers: - Mucosa- Submucosa- Muscularis propria (externa)- Subserosa• Serosa - contains mesothelial lining, loose connective tissue
• Lamina propria: contains loose connective tissue, lymphocytes, plasma cells, occasional eosinophils, macrophages, mast cells, neutrophils
Mucosa
• contains villi with central blood vessels, lymphatics
• epithelium• lamina propria• muscularis mucosa
Mucosa
• Villi: contain microvilli; contain primarily columnar absorptive cells and goblet cells
• Absorptive cells: have microvilli on luminal surface (brush border) and underlying mat of microfilaments (terminal web)
Crypts of Lieberkuhn• lower 20% of epithelium, contain
undifferentiated (immature) crypt cells, Paneth cells (have large, apical eosinophilic granules containing antimicrobial proteins), scattered goblet cells and endocrine cells
• secrete ions, water, IgA, antimicrobial peptides into lumen
• crypt cells take 3-8 days to migrate to surface; allows for rapid repair, but also causes these cells to be sensitive to radiation therapy and chemotherapy
Muscularis propria (externa) inner circular and
outer longitudinal layer, with myenteric (Auerbach’s) plexus between these layers; plexus also contains interstitial cell of Cajal, ganglion cells, fibroblasts
Auerbach’s cells
• Interstitial cell of Cajal =type of interstitial cell found in the gastrointestinal tract that serves as a pacemaker which creates the basal electrical rhythm leading to peristalsis
• ganglion cells=special nerve cells in the intestine that make the muscles push; congenital aganglionosis-Hirschsprung's disease
• fibroblasts=produce the extracellular matrix and participate in the transport of absorbet metabolites to the blood and lymphatic apillaries
Endocrine cells• similar to cells in pancreas,
biliary tree, lung, thyroid, urethra
• contain fine eosinophilic granules with secretory proteins
• nuclei on luminal side of granules, not basal
- Serotonine (enterocromafine)- Gastrine (G)- Secretine (S)- Enteroglucagon (EG)
Congenital anomalies
• Meckel diverticulum• Duplications• Intestinal atrezia & stenosis• Malrotation• Gastroschisis & omphalocele
Meckel diverticulum
• During early gestation, the omphalomesenteric or vitelline duct connects the fetal yolk sac to the primitive gut. By 7 to 8 weeks of gestation, this duct is normally completely obliterated.
• A Meckel diverticulum, results when this structure fails to resorb completely.
Symptoms
• most adults remain asymptomatic• intestinal obstruction is manifested by cramping
abdominal pain, obstipation, nausea and vomiting • acute Meckel's diverticulitis is characterized by
abdominal pain and tenderness typically localized below or to the left of the umbilicus; it is often accompanied by vomiting and is similar to appendicitis except for location of pain.
• bleeding- typically resulting in melena rather than frank blood.
Signs
• voluntary guarding with mild tenderness - in the absence of strangulation, the abdomen is not tender- with infarction, the abdomen becomes tender and
auscultation reveals a silent abdomen or minimal peristalsis• hyperactive, high-pitched peristalsis with rushes coinciding
with cramps is typical• sometimes, dilated loops of bowel are palpable• shock and oliguria are serious signs that indicate either late
simple obstruction or strangulation
Diagnosis
• based on symptoms• flat and upright X rays of the abdomen ‑ (vomiting and
signs of obstruction) • CT scan with oral contrast (for abdominal pain and
focal tenderness)• wireless capsule• radionuclide scan - 99mTc pertechnetate scan may identify ectopic gastric
mucosa and hence the diverticulum (if rectal bleeding is suspected to originate from a Meckel's diverticulum)
Axial contrast-enhanced CT scan shows blind-ending Meckel's diverticulum with thickened mucosal folds (arrow). Pathology confirmed ectopic gastric mucosa in Meckel's diverticulum.
Giant Meckel diverticulum in a 21-year-old man who was referred for wireless capsule endoscopy because of chronic abdominal pain and anemia. Results of a small bowel follow-through study, radionuclide examination, and endoscopy of the upper and lower gastrointestinal tract were unremarkable. (a) Wireless capsule endoscopic image shows a shallow ulcer in one segment of the ileum (arrow). Other images showed ulcers in an adjacent segment and possibly in the colon. Double-contrast barium enteroclysis was requested to determine the extent of Crohn disease. (b) Double-contrast air-barium enteroclysis image shows a large saccular dilatation (arrowheads) in a pelvic segment of the ileum. Scattered ulcerations (arrow) are seen adjacent to the point of attachment of the dilatation to a normal-appearing loop of ileum. Results of surgery confirmed the presence of a giant Meckel diverticulum with ulcerations. There was no evidence of Crohn disease.
Technetium-99m pertechnetate scan in a 12-year-old boy who presented with intermittent dull abdominal pain and a mild iron deficiency anemia. On the present occasion, the pain appeared more severe and was associated with occasional vomiting; thus, the child was hospitalized. This 90-minute delayed image shows focal activity in the mid abdomen. The activity is more diffuse than is expected with Meckel diverticulum.
At surgery, an inflamed Meckel diverticulum containing ectopic gastric mucosa was removed.
The Meckel diverticulum had intussuscepted into the terminal small bowel.
Differential diagnosis
• appendicitis• intestinal polyposis syndromes• colitis• intussusception• colonic vascular malformations• juvenile polyps• necrotizing enterocolitis• Crohn disease• ulcerative colitis
Complications
• The risk for complications dramatically decreases with age, and most adults with a Meckel diverticulum remain asymptomatic.
• Complications develop in approximately 2% of all adults with a Meckel diverticulum:
- bleeding- intestinal obstruction- diverticulitis- perforation- carcinoma
Obstruction is caused by:
• intussusception of the diverticulum into adjacent bowel
• volvulus around or herniation into a fibrous band
• entrapment in inguinal, femoral or umbilical hernia sacs (Littré hernia)
• inflammation and scarring leading to blockage around the diverticular neck and adjacent ileum
Volvulus
• abnormal twisting of the intestine around the axis of its own mesentery, resulting in obstruction of the more proximal bowel
• twisting of the mesentery may involve the mesenteric vessels and so make the involved loop particularly susceptible to strangulation and gangrene, with resulting perforation, peritonitis and sepsis
Symptoms
• often has an abrupt onset
- abdominal pain - continuous, sometimes with superimposed waves of colicky pain
- obstipation- nausea- vomiting - marked abdominal
distention
Signs
• abdominal distention• rebound• guarding • rigidity• a palpable abdominal
mass (occasionally)
Complications
• SURGICAL EMERGENCY!
• strangulation of the twisted bowel loop• loss of blood supply• deterioration• perforation• fatal peritonitis when the bowel material
infects the abdominal cavity
Investigations
• abdominal and chest X-rays may show the obstruction and abnormal air-fluid levels in the bowels
• barium enema X-ray shows typical volvulus shapes
• CT• white blood cell count will be higher than
normal
Radiological investigations
• Plain abdominal radiographs taken in supine and upright positions may demonstrate distended bowel with air-fluid levels, consistent with obstruction.
• Perforation may be indicated by the presence of free air.
• A typical corkscrew-like appearance of the barium in the distorted duodenum and jejunum is diagnostic.
• Angiography may reveal twisting of the branches of the superior mesenteric artery.
Dysmotility
• Chronic small intestine pseudoobstruction- it may be secondary to neuropathy or
myopathy- abnormalities of small bowel ICCs- there is some evidence of a genetic
association - it can occur in conjunction with Kawasaki
disease or Parkinson's disease
Dysmotility-causes
Primary • Familial visceral myopathies• Mithocondrial DNA and
myopathies• Familial visceral neuropathies• Congenital neuropathic motility
disorders• MEN type 2B• Non-familial visceral
myopathies• Idiopatic non-familial visceral
neuropathies
Secondary • Scleroderma • Dermatomyositis and polymyositis• Systemic lupus erythematosus• Mixed connective tissue disease• Diabete mellitus• Parkinson disease• Neurofibromatosis• Spinal cord injury• Paraneoplastic visceral neuropathy• Myotonic distrophy• Amiloidosis• Thyroid disease• Hypoparathyroidism• Drug-induced changes in small intestine
motility• Celiac disease• Irradiation
Clinical findings
• Isolated severe small intestinal dysmotility is very unusual; small intestinal dysmotility is generally associated with dysmotility in other parts of the digestive tract.
• asymptomatic• recurrent symptoms and signs of small
intestinal obstruction = chronic small intestinal pseudoobstruction
Symptoms • Between those two ends of the spectrum, the patient may have recurrent
symptoms - postprandial cramping- periumbilical and epigastric abdominal pain- abdominal bloating - easy satiety - anorexia- weight loss - nausea- vomiting
• symptoms are usually related to eating. • diarrhea can occur in patients with bacterial overgrowth and malabsorption. • in severe cases, the patients have episodes of chronic intestinal
pseudoobstruction syndrome
Signs
• cachectic and malnourished• the abdomen may be distended and mildly tender• the bowel sounds are inactive and infrequent in patients
with smooth muscle dysfunction, but they are hyperactive and high-pitched in those with myenteric plexus dysfunction
• in those with chronic intestinal pseudoobstruction, during an obstructive episode, the abdominal examination findings may be indistinguishable from those of true mechanical obstruction
• symptoms and signs of multiple-organ dysmotility
Complications
• malnutrition• bacterial overgrowth• pneumatosis cystoides intestinalis - rare condition
characterized by multiple, gas-filled cysts in the wall of the small and large intestine. Pneumoperitoneum may occur.
Investigations
• Blood tests• Plain abdominal X-ray• Enteroclysis• Whole-gut transit with radiopaque markers• Radioactive isotope transit by scintigraphy• Small intestinal manometry
Blood tests
• Blood cell count: anemia and macrocytosis
• Blood chemistries: malnutrition, malabsorption
Plain abdominal X-ray
• during exacerbations, show multiple air-fluid levels and dilation of the small intestine
Enteroclysis
Spot radiograph of small intestine from enteroclysis shows marked dilation of the mid small intestine. The luminal diameter is 9 cm (double arrow). Despite the marked luminal dilation, the valvulae conniventes are tightly packed. The folds are smooth and of normal caliberScleroderma (Small Bowel)
Differential diagnosis between chronic intestinal pseudoobstruction and mechanical obstruction
• Partial small bowel obstruction from adhesions, tumors, intussusception or stricture can mimic chronic intestinal pseudoobstruction.
• Enteroclysis or careful small bowel radiography with fluoroscopy is probably the most helpful way to differentiate chronic intestinal pseudoobstruction from mechanical obstruction.
• In most cases, exploratory laparoscopy may be necessary to rule out an obstructing lesion.
Infections
Acute• Common bacteria• Viral pathogens• Traveller’s diarrhea
Chronic • Whipple disease• Tropical sprue• Tuberculosis• Mycotic infections
Pathophysiology
Host factors
• Normal intestinal flora• Control mechanisms• Intestinal immunity
Microbial factors
• number of organisms
• enterotoxins• adherence to gut mucosa• invasion of enterocytes
Clinical manifestations
• Diarrhea• Nausea and vomiting• Loss of appetite• Fever• Headaches• Abnormal flatulence• Abdominal pain• Bloody stools (dysentery - suggesting infection by
amoeba, Campylobacter, Salmonella, Shigella or some pathogenic strains of Escherichia coli)
Diagnosis • diagnosing gastroenteritis is mainly an exclusion procedure
• in rare cases when the symptoms are not enough to diagnose gastroenteritis, several tests may be performed in order to rule out other gastrointestinal disorders.
- rectal examinations- complete blood count- electrolytes- kidney function tests
• when the symptoms are conclusive, no tests apart from the stool tests are required
Diarrhea - the most common manifestation of intestinal tract infections
• Young children and the elderly are at greatest risk for more severe disease and complications.
• The presence of underlying medical conditions, especially those that compromise immunity, greatly enhances the risk of acquiring an infection and its ultimate severity.
• Poor sanitation, inadequate water supplies and increasing globalization of food transport systems all predispose to the development of large epidemics of food- and water-borne outbreaks of gastrointestinal disease.
• Seasonal or cyclic weather variations also influence the epidemiology of diarrhoeal disease and food poisoning.
Is just a little case of diarrhea…
• Second leading causes of all death worldwide
• Most common cause of morbidity and mortality in children worldwide
• Accounts for 9% of hospitalizations in children <5 years old in the United States
• You will likely suffer from diarrhea in the near future!
Definition
• >3 feces/day, > 200 g/day• acute/chronic
• Physiology:– in gastrointestinal tract 9-10 l fluids (2l ingestion,
the rest secretions);– Na - co-transport with Cl and glucose in small
bowel and biliary salts in terminal ileum; co-transport with H - HCO3; K absorbed with H or Ca.
– parasimpatic is stimulating the peristalsis and electrolyte secretion; simpatic nerves are doing the opposite.
– enteric nervous system
Acute diarrhea - definition
• Stool weight in excess of 200 g/day
• 3 or more loose or watery stools/day
• Alteration in normal bowel movement characterized by decreased consistency and increased frequency
• Less than 14 days in duration
Etiology
• Viral: 70-80% of infectious diarrhea in developed countries
• Bacterial: 10-20% of infectious diarrhea but responsible for most cases of severe diarrhea
• Protozoars: less than 10%
Epidemiology
• 1.2-1.9 episodes per person annually in the general population
• 2.4 episodes per child <3 years old annually• 5 episodes per year for children <3 years old
and in daycare• Seasonal peak in the winter
Rotavirus
• Leading cause of hospitalization for diarrhea in children
• Most prevalent during winter season
• Fecal-oral transmission: viral shedding can persist for 21 days
• Acute onset of fever followed by watery diarrhea (10-20 BM/day) and can persist for up to a week
Norovirus
• Most common cause of diarrheal outbreaks/epidemics
• Multiple modes of fecal-oral transmission• Acute onset of nausea and vomiting, watery
diarrhea with abdominal cramps and can persist for 1-3 days
Enteric adenovirus
• Primarily affects children < 4 years old
• Fecal-oral transmission
• Clinical picture similar to rotavirus (fever and watery diarrhea)
Astrovirus
• Primarily affects children < 4 years old and immunocompromised
• Seasonal peak in the winter
• Fecal-oral transmission: viral shedding can occur for several weeks
• Fever, nausea and vomiting, abdominal pain and diarrhea lasting up to a week
Symptoms of viral enteritis
• low grade fever
• nausea
• vomiting
• abdominal cramps
• watery diarrhea lasting up to 1 week
• Viral shedding can occur for weeks after symptoms resolve
Campylobacter
• Most common bacterial pathogen
• Transmitted through ingestion of contaminated food or by direct contact with fecal material
• diarrhea (+/- blood), abdominal cramps (can be severe), malaise, fever
• Usually self-limited and does not require antibiotics
Salmonella
• Most common in children <4 years old and a peak in the first few months of life
• Transmitted via ingestion of contaminated food and contact with infected animals
• fever, diarrhea and abdominal cramping• Antimicrobial therapy can prolong fecal shedding
Shigella
• Fecal-oral transmission• fever, abdominal cramps, tenesmus, and
mucoid stools with or without blood• Can lead to serious complications • Antimicrobial treatment shortens duration of
illness and limits fecal shedding
E. Coli O157:H7
• Transmission via contaminated food and water
• bloody diarrhea, severe abdominal pain, and sometimes fever
• Can lead to serious complications
• Antibiotics have no proven benefit and may increase the risk of complications
Symptoms of bacterial enteritis
• Can affect all age groups
• Fecal-oral transmission, often through contaminated food
• bloody diarrhea, severe cramping and malaise
• Antibiotic treatment not always necessary
History and Physical Exam
• 3 main goals– Estimate the level of dehydration
– Identify likely causes on the basis of history and clinical findings
– Determine if additional studies and/or medications are necessary
History
• Onset, frequency, quantity, and character of diarrhea
• Associated symptoms: nausea, vomiting, fever, abdominal pain, tenesmus, malaise
• Recent oral intake• Signs and symptoms of dehydration
Tenesmus
• Tenesmus is the feeling that you constantly need to pass stools, even though your bowels are already empty.
• It may involve straining, pain, and cramping.
• Usually occurs with inflammatory diseases of the bowels.
• It can also occur with motility disorders.
Malaise
• Malaise is a generalized feeling of discomfort, illness or lack of well-being.
• Malaise is a symptom that can occur with almost any significant health condition.
• It may start slowly or quickly, depending on the type of disease.
• Fatigue occurs with malaise in many common diseases. Mailaise can be accompanied by a feeling of not having enough energy to accomplish usual activities.
Physical Exam
• Vitals, vitals, vitals!
• Abdominal exam
• Presence of occult blood
• Signs of dehydration
Dehydration • particularly dangerous in children, older adults and people with
weakened immune systems• must be treated promptly to avoid serious health problems, such as
organ damage, shock or coma
• thirst• less frequent urination than usual• dark-colored urine• dry skin, does not flatten back to normal right away after being gently
pinched and released• fatigue• dizziness• light-headedness
Laboratory evaluation
• Unnecessary for patients who present within 1 day from onset of diarrhea
• Warning signs/symptoms: bloody diarrhea, high fever, severe abd pain, dehydration or comorbid condition
• Fecal leukocytes followed by bacterial culture, ova & parasites, viral antigens
• CBC, chemistries
TRAVELER’S DIARRHEA
• substantial risk (~40%) for diarrheal disease• To some degree, the specific agents that cause traveler’s
diarrhea vary by geographic region and season. • Giardia and Cryptosporidium appear to be common causes
of diarrheal disease in visitors to Russia• Aeromonas spp appear to be very common causes of
traveler’s diarrhea in visitors to Thailand• toxigenic E coli is somewhat more frequently encountered
during the warmer summer months• Campylobacter jejuni appears to occur more frequently in
the winter months
Clinical features
• Traveler’s diarrhea usually occurs within the first 14 days of travel.
• It can also occur within a week or more after return from a foreign country.
• The diarrhea is usually characterized as watery, with the passage of three to ten bowel movements a day for 2 to 5 days.
• Abdominal cramps and pain often accompany the illness.• Fewer patients experience fever, chills, vomiting and
dysentery-like symptoms. • Fewer than 10% of patients have an illness that lasts longer
than a week and about 2% of patients have illness lasting a month or more
Diagnosis
• Rarely is diagnosis required or available in the setting of acute watery traveler’s diarrhea.
• For cases of dysentery, a diagnosis, if available, is more useful.
• Given that traveler’s diarrhea occurs in the traveling patient, it is almost always reasonable to initiate treatment without an etiologic diagnosis.
• Stool examination for parasites is warranted only in cases of prolonged illness.
Chronic diarrhea - definition
• >3 weeks duration• usually means three or more loose stools per
day• average fecal daily weight in normal person is
100-200grams/day
Approach to patient
• Patient should be questioned about the onset, duration, pattern, aggravates (especially diet), relieving factors and stool characteristics
• Presence or absence of fecal incontinence, fever, weight loss, pain, certain exposures-travel, medications, contacts with diarrhea should be noted
Approach to patient
• On physical exam, check for thyroid mass, wheezing on lung exam, heart murmurs, edema, hepatomegaly, abdominal mass, LAD, perianal fistula or anal sphincter laxity.
• If diagnosis is still unclear after initial encounter, further testing is required
• secretory vs. osmotic diarrhea vs. malabsorption vs. inflammatory
Tests
• Stool culture - a sample of stool is analyzed in a laboratory to check for bacteria, parasites, or other signs of disease and infection.
• Blood tests - can be helpful in ruling out certain diseases.
• Fasting tests - to find out if a food intolerance or allergy is causing the diarrhea, the doctor may ask a person to avoid foods with lactose, carbohydrates, wheat, or other ingredients to see whether the diarrhea responds to a change in diet.
Complications
• Dehydration• Malnutrition• Electrolytes (minerals) deficiencies• Finally, there may be irritation of the anus due
to the frequent passage of watery stool containing irritating substances
Malabsorptive diarrhea
• Malabsorption suspected in patients with weight loss, greasy stools, glossitis, anemia and hypoalbumenima
• If malabsorption suspected, a 72 hr stool specimen should be sent for fecal fat determination, if + =>suspect malabsorption
• Causes of malabsorption include pancreatic insufficiency (confirmed by CT/pancreatic function tests) and disease of small intestine--Whipple’s disease, tropical sprue, intestinal lymphoma (small bowel biopsies by EGD)
Malabsorptive Diarrhea-Mucosal Malabsorbtion
• Celiac sprue - hypersensitivity to gluten• Tropical sprue - infectious disease of unknown
origin, seen in Indian subcontinent, Asia, West Indies, North & South America, central and southern Africa, and Central America
Mucosal Malabsorptive
• Whipple’s ->infection form Treponema-whippelii.
• Diagnosed by + biopsy for PAS macrophages• Associated symptoms include
hypersomnolescence, arthralgias, fever, hypotension and LAD
Intraluminal Malabsorbtion
• Most commonly results from pancreatic exocrine insufficiency when >90% of pancreatic secretory function is lost
• ethanol abuse• cystic fibrosis• pancreatic duct obstruction
Secretory vs Osmotic
• check stool osmotic gap• 290-2x[Na stool + K stool]• If < 50, diarrhea falls under secretory category
TYPICAL FEATURES OF SECRETORY DIARRHEA
TABLE 4-5. TYPICAL FEATURES OF SECRETORY DIARRHEA
Voluminous, watery stools
Little or no fecal osmotic gap, stool pH near 7.0
Usually persists during fasting
Usually no pus, blood, or excess fat in stools
Secretory Diarrhea
• Characterized by watery, large-volume fecal outputs that are typically painless and persist with fasting - one may do a 24 hr stool quant.
-should exceed one liter and not decrease with fasting
• Usually stool pH is neutral and fecal fat test is negative
TABLE 4-6. MECHANISMS AND CAUSES OF SECRETORY DIARRHEA
Reduction in mucosal surface area
Postresection diarrhea
Short-bowel syndrome
Extensive mucosal disease and Inflammation
Viral gastroenteritis
Celiac disease
Whipple s̀ disease
Crohn s̀ disease
Lymphoma
Absence of ion transport mechanism
Congenital chloridorrhea
Bacterial toxins
Cholera
Enterotoxigenic Escherichia coli
Shigella
Staphylococcus
Clostridium perfringens
Luminal secretagogues
Bile acids
Fatty acids, hydroxy-fatty acids
Phenolphthalein, ricinoleic acid, bisacodyl
Circulating secretagogues
Gastrin (Zollinger-Ellison syndrome)
Vasoactive intestinal polypeptide (VIPoma, ganglioneuroma, neuroblastoma, pheochromocytoma)
Calcitonin, prostaglandins (medullary carcinoma of the thyroid)
Somatostatin (somatostatinoma)
Glucagon (glucagonoma)
Serotonin, kinins (carcinoid tumor)
Thyroxine (hyperthyroidism)
Histamine (mastocytosis)
Secretory diarrhea - investigations
• If secretory diarrhea confirmed, recommend checking serum should be sent for:
• Gastrin (gastrinoma), VIP(VIPOMA), glucagon (glucogonoma), serotonin (carcinoid), calcitonin, histamine, and prostaglandins
• -if overproduction of one of these mediators is documented abdominal CT scan is recommended
Carcinoid Syndrome and Secretory Diarrhea
• Carcinod present with watery diarrhea, flushing, skin changes, bronchospasm and cardiac murmurs which are all symptoms caused by secretion of serotonin, histamine, catecholamines, kinins and prostaglandins by the tumor masses
• 1/3 pts with carcinoid present with diarrhea alone
Sectretory diarrhea – differential diagnosis
• Other conditions to consider include:• Diseases like Crohn’s ileitis or resection of
<100cm of terminal ileum (dihydroxy bile acids may escape absorption and stimulate colonic secretion)
Osmotic Diarrhea
• Most common cause is lactase deficiency• Magnesium ingestion or factitious laxative
abuse• Intraluminal maldigestion is also seen in
cirrhotics and bile duct obstruction-there is impaired delivery of bile salts to small intestine, leads to poor micelle formation with ingested fats
CHRONIC DIARRHEA -Investigation-
• Blood tests: ESR; hemo leucograme (anemia, inflammation); proteinograme (hyposerinemia)
• Rectosigmoidoscopy, Colonoscopy with/without biopsy/ UGI endoscopy ( differential diagnosis )
• Rx: small bowel/barium enema
• Chronic diarrhea: Abdominal X-Ray, US/ CT
Celiac disease
• Coeliac disease is an inflammatory disorder of the small intestine induced by the prolamins of certain cereals, namely the gliadins of wheat, hordeins of barley and secalins of rye.
• The inflammation is associated with loss of villous height and crypt hypertrophy and leads to malabsorption.
(a) Dissecting microscopic appearance of a normal jejunal biopsy. (b) Dissecting microscopic appearance of coeliac disease.
Pathogenesis
• There are two clear facts about the etiopathogenesis of coeliac disease.
1. The first is that fractions of gliadin, the alcohol-soluble component of gluten, are the toxic dietary constituent, together with similar fractions of rye and barley prolamins.
2. The second is that there is a genetic susceptibility to gluten intolerance because of the close association with the HLA haplotype B8-DR3-DQ2 in northern Europeans and with B8-DR5/7-DQ2 in southern Europeans.
Clinical findings
• Coeliac disease in infants classically presents soon after weaning at the point that cereals are introduced.
• In adults, the most common presentations are anaemia and variable abdominal symptoms of discomfort, bloating, excess wind and an altered bowel habit (diarrhea). Mouth ulcers are also frequent and can be the presenting symptom.
Diagnosis
• The crucial test to establish the diagnosis is a small-intestinal biopsy.
• Several serological tests have been developed as screening tests
- antibodies to gliadin (IgA or IgG isotype)- IgA antibodies to reticulin- IgA antibodies to endomysium
Diagnosis
• Assessment of malabsorption
• Full blood count (hemoglobin level may be low, folate deficiency, vitamine B12 - concentrations
• are only low in patients with extensive involvement of the small intestine and so are usually normal)
• Biochemistry – hypokalaemia, hypomagnesiemia, hypocalcaemia, serum albumin is often low, as is the concentration of zinc; faecal fat excretion
• Immunological tests• Radiology• Small-intestinal biopsy
Small intestinal biopsy
• This has traditionally been taken from the duodenal–jejunal junction (the ligament of Treitz) using a Crosby capsule.
• a distal duodenal biopsy taken at endoscopy is being used increasingly to make the diagnosis and comparative studies with a true jejunal biopsy have justified its use.
Differential diagnosis
• Giardia• common-variable hypogammaglobulinaemia• Lymphoma• Crohn's disease• small-intestinal diseases such (radiation,
enteritis, amyloid, Whipple's disease)• Dermatitis herpetiformis is commonly
associated with an abnormal mucosal biopsy
Associated diseases
• There is an increased prevalence of autoimmune diseases in patients with coeliac disease:
• diabetes• thyroid disease• Addison's disease• fibrosing alveolitis• systemic lupus erythematosus• polyarteritis
Short bowell syndrome
• Large resections of the small bowel may cause multiple nutritional and other medical abnormalities, now commonly termed the 'short bowel syndrome'.
• thrombosis or embolus• multiple surgical resections of the small bowel
in patients with Crohn's disease (regional ileitis)
Clinical findings
• Intractable (cholerheic) diarrhoea• Steatorrhoea• Consequential metabolic abnormalities including
vitamin B 12 deficiency • Many patients undergoing resections will be
malnourished preoperatively and energy consumption increases in the immediate postoperative period.
• If not appropriately managed, long-term protein-energy malnutrition, as well as life-threatening mineral and vitamin deficiencies develop.
Adaptation
• The residual bowel undergoes mucosal hyperplasia and its capacity to absorb fluids and nutrients increases over a period of weeks or months.
• The molecular events that underly these changes are unclear but may include circulating trophic factors and growth factors present in pancreatic juice or secreted into the intestinal lumen.
CONSTIPATION
1. Definition2. Pathogenesis3. Risk factors4. Diagnosis and differential diagnosis5. Treatment approaches
Definition: usually refers to persistent, difficult, infrequent or seemingly incomplete defecation
The patient’s view:
The following perceptions,
• Need for straining (52%)
• Hard pellet-like stools (44%)
• Inability to defecate when desired (34%)
• Infrequent defecation (33%)
The clinical view: ROME-CRITERIA (at least 2 in any 12week period);
• < 3 bowel movements (BM) per week
• Hard stools in > 25% of BM’s
• Sense of incomplete evacuation in >25% of BM’s
• Excessive straining in >25% of BM’s
• The necessity of digital manipulation
2. Causes
•Extrinsic
• Inadequate dietary fiber, fluid
• Ignoring urge to defecate
•Structural
• Colorectal: neoplasm,stricture,ischemia,volvulus,diverticular disease
• Anorectal: inflammation, prolapse, rectocele,fissure, stricture
•Systemic
• Hypokalemia
• Hypercalcemia
• Hyperparathyroidism
• Hypothyroidism
• Diabetes mellitus
• Addison’s disease
• Pregnancy
• Uremia
•Neurological
• CNS: Parkinson's disease, Multiple sclerosis, trauma, ischemia, tumor
• Sacral nerves: trauma, tumor
• Autonomic neuropathy
• Aganglionosis ( Hirschsprung’s disease )
•Drugs
• Analgesics
• Anticholinergics
• Anticonvulsants
• Antihistamines
• Antihypertensive
• Chemotherapeutic agents
• Diuretics
• Metal ions
•Uncertain Pathophysiology
Irritable bowel syndrome, Slow transit constipation (STC)
3. Risk factors
Risk situations, groups and factors:
• Infants and children
• People older than 55 yrs
• Recent abdominal or perianal/pelvic surgery
• Late pregnancy
• Limited mobility
• Inadequate diet (fluid or fiber)
• Medications especially in the elderly
• Laxative abuse
• Terminal care patients
• Travel
• History of chronic constipation
4. Diagnosis and differential diagnosis
• History taking
• Physical examination
• Diagnostic techniques
• History taking
•Check for age of onset ( sudden or long term)
•Check for ROME- II criteria
•Check for neurological disorders
•Check for psychiatric conditions
•Check for family history of constipation?
• Physical examination
•Palpation of abdomen ( tumour )
•Percussion ( check for gases)
•Rectal palpation
• Consistency/impaction
• Presence of non-fecal masses or abnormalities (tumors, hemorrhoid, fissures)
• Presence of blood
• Sphincter tone
Major alarm symptoms especially in patients >50yrs
•New onset constipation
•Anemia
•Weight loss
•Anal blood loss
•Positive occult blood test
•Sudden changes in defecation pattern and appearance of stool
• Diagnostic techniques
•Stool analysis
• Weighing 3 days; < 100g avg means constipation
•Abdominal x-rays
•Radiological or endoscopic investigation
• Colon tumour, stenosis
•Abdominal echography
• Tumour mass
•Anorectal function tests
• Manometry
• Electromyography
•Rectal mucosal biopsy
•Colonic transit time (radiopaque marker)
Clinical term that encompasses defects occurring during the digestion and absorption of food nutrients by the gastrointestinal tract.
• The digestion or absorption of a single nutrient component may be impaired, as in lactose intolerance in lactase deficiency.
• When a diffuse disorder such as celiac disease affects the intestine, the absorption of almost all elements is impaired.
MALABSORPTION – definition
Pathophysiology:
3 major phases of digestion and absorption of food materials.
• Luminal phase: dietary fats, proteins, and carbohydrates are hydrolyzed and solubilized by secreted digestive enzymes and bile.
• Mucosal phase: relies on the integrity of the brush-border membrane of intestinal epithelial cells to transport digested products from the lumen into the cells.
• Post absorptive phase: reassembled lipids and other key nutrients are transported via lymphatic and portal circulation from epithelial cells to other parts of the body.
Symptoms • Diarrhea
– Diarrhea is the most common symptomatic complaint.– Diarrhea frequently is watery, reflecting the osmotic load received by
the intestine.– Bacterial action producing hydroxy fatty acids from undigested fat also
can increase net fluid secretion from the intestine, further worsening the diarrhea.
• Steatorrhea– Steatorrhea is the result of fat malabsorption. – The hallmark of steatorrhea is the passage of pale, bulky, and
malodorous stools. – Such stools often float on top of the toilet water and are difficult to
flush. Also, patients find floating oil droplets in the toilet following defecation.
Symptoms • Weight loss and fatigue
– Weight loss is common and may be pronounced; however, patients may compensate by increasing their caloric consumption, masking weight loss from malabsorption.
– The chance of weight loss increases in diffuse diseases involving the intestine, such as celiac disease and Whipple disease.
• Flatulence and abdominal distension– Bacterial fermentation of unabsorbed food substances releases
gaseous products, such as hydrogen and methane, causing flatulence. – Flatulence often causes uncomfortable abdominal distention and
cramps.
Symptoms • Edema
– Hypoalbuminemia from chronic protein malabsorption or from loss of protein into the intestinal lumen causes peripheral edema.
– Extensive obstruction of the lymphatic system, as seen in intestinal lymphangiectasia, can cause protein loss.
– With severe protein depletion, ascites may develop.• Anemia
– Depending on the cause, anemia resulting from malabsorption can be either microcytic (iron deficiency) or macrocytic (vitamin B-12 deficiency).
– Iron deficiency anemia often is a manifestation of celiac disease. – Ileal involvement in Crohn disease or ileal resection can cause
megaloblastic anemia due to vitamin B-12 deficiency.• Bleeding disorders
– Bleeding usually is a consequence of vitamin K malabsorption and subsequent hypoprothrombinemia.
– Ecchymosis usually is the manifesting symptom, although occasionally, melena and hematuria occur.
Symptoms • Metabolic defects of bones
– Vitamin D deficiency can cause bone disorders such as osteopenia or osteomalacia.
– Bone pain and pathological fractures may be observed. – Malabsorption of calcium can lead to secondary hyperparathyroidism.
• Neurological manifestations– Electrolyte disturbances such as hypocalcemia and hypomagnesemia
can lead to tetany, manifesting as the Trousseau sign and the Chvostek sign.
– Vitamin malabsorption can cause generalized motor weakness (pantothenic acid, vitamin D) or peripheral neuropathy (thiamine), a sense of loss for vibration and position (cobalamin), night blindness (vitamin A), and seizures (biotin).
Physical findings• General
– Patients may have orthostatic hypotension. – Fatigue– Signs of weight loss, muscle wasting, or both may be
present.– Patients may have signs of loss of subcutaneous fat.
• Abdominal examination– The abdomen may be distended, and bowel sounds may
be hyperactive.– Ascites may be present in severe hypoproteinemia.
• Dermatological manifestations– Pale skin may reveal anemia.– Ecchymosis due to vitamin K deficiency may be
present.– Dermatitis herpetiformis, erythema nodosum, and
pyoderma gangrenosum may be present. – Pellagra, alopecia, or seborrheic dermatitis
• Neurological examination– Motor weakness, peripheral neuropathy, or ataxia may
be present.– The Chvostek or Trousseau sign may be evident due to
hypocalcemia or hypomagnesemia.• Cheilosis, glossitis, or aphthous ulcers of the
mouth• Peripheral edema
TABLE 5-33. SELECTED SYMPTOMS AND SIGNS OF NUTRIENT DEFICIENCIESSymptoms or sign Possible nutrient deficiency
Weakness, weight loss, musclewasting
Protein, calorie
Pallor Folate, iron, vitamin B12
Follicular hyperkeratosis Vitamin A, vitamin CPerifollicular petechiae Vitamin C
DermatitisProtein, calorie, niacin, riboflavin, zinc,vitamin A, essential fatty acids
Bruising, purpuraEasily plucked, alopecia Vitamin C, vitamin KCorkscrew hairs, coiled hair Protein, zinc, biotin
Night blindness, keratomalacia,photophobia
Vitamin C, vitamin A
Conjunctival inflammation Vitamin AGlossitis Vitamin A, riboflavinBleeding or receding gums, mouthulcers
Riboflavin, niacin, folate, vitamin B12,protein
Decreased taste Vitamin A, vitamin C, vitamin K, folateBurning or sore mouth and tongue Zinc, vitamin A
Angular stomatitis or cheilosisVitamin B12, vitamin C, niacin, folate,iron
Tetany Riboflavin, niacin, pyridoxine, ironParesthesias Calcium, magnesiumLoss of reflexes, wrist drop, foot drop,loss of vibratory and position sense
Thiamine, pyridoxine
Vitamin B12, vitamin EDementia, disorientation Niacin, vitamin B12
Ophthalmoplegia Vitamin E, thiamineDepression Biotin, folate, vitamin B12
TABLE 5-1. CLASSIFICATION OF DISEASES THAT CAUSEINTESTINAL MALABSORPTION
Premucosal Mucosal Postmucosal
Pancreaticinsufficiency
Celiac sprueCongenitallymphangiectasia
Hepatobiliarydisease
Tropical sprueSecondarylymphangiectasia
Bacterialovergrowth
Whipple`s disease
Rapid intestinaltransit
Eosinophilic enteritis
GastrectomyBrush border enzymedeficiency
Lymphoma
Short-bowel syndrome
Prolonged malnutrition
Radiation enteritis
Parasitic infection
Mesenteric ischemia
Massive small-bowel resection can cause significant malabsorption
TABLE 5-16. PREDICTED NUTRITIONAL OUTCOME IN PATIENTS WHO HAVE HAD MASSIVEINTESTINAL RESECTION
Remaining Jejunal length, cm Colon Nutritional outcome
0-50 - TPN
+ TPN
51-100 - IVFM/TPN
+ Modified oral diet
101-150 - Regular or modified oral diet
+ Regular diet
151-200 - Modified oral diet
+ Regular diet
>200 - or + Regular diet
©Copyright Science Press Internet Services
Differentials:
• Zollinger-Ellison Syndrome
Other Problems to be Considered: – Amino acid deficiencies (cystinuria)– Cystic fibrosis– Hartnup disease– Tropical jejunitis– Whipple disease
TABLE 5-32. INITIAL EVALUATION OF PATIENT WITH POSSIBLEMALABSORPTION
History and Physical ExaminationInitial blood tests Follow-up laboratory tests
Complete blood count Serum ironProthrombin time Serum folateStandard electrolytes Serum vitamin B12
Calcium Serum vitamin AMagnesium Plasma 25-hydroxy vitamin DBlood urea nitrogen Urinary oxalate excretionCreatinine Stool for Sudan stainAlkaline phosphatase Stool for ova and parasitesCholesterolTotal protein and albumin
Workup :
Imaging studies
– Small bowel barium studies.– CT-scan of the abdomen. – Endoscopic retrograde cholangiopancreatogram– Plain abdominal X-ray film. – Endoscopy
Endoscopy Upper endoscopy with small bowel mucosal biopsy
• Establishing a definitive diagnosis of malabsorption of the mucosal phase often can be achieved by histological examination of biopsied mucosal specimens obtained during routine upper endoscopy.
• Examples of conditions that can be diagnosed this way include celiac sprue, giardiasis, Crohn disease, Whipple disease, amyloidosis, abetalipoproteinemia, and lymphoma.
Endoscopic image of scalloping seen in celiac disease and other mucosal disorders including giardiasis
Other studies
– Tests of fat malabsorption.– D-xylose test. – Test of carbohydrate absorption. – Test of bile salt absorption. – Schilling test.
URINARY D-XYLOSE TEST • The urinary D-xylose test for carbohydrate absorption provides
an assessment of proximal small-intestinal mucosal function. D-Xylose, a pentose, is absorbed almost exclusively in the proximal small intestine.
• The D-xylose test is usually performed by giving 25 g D-xylose and collecting urine for 5 h.
• An abnormal test (4.5 g excretion) primarily reflects the presence of duodenal/jejunal mucosal disease.
• The D-xylose test can also be abnormal in patients with blind loop syndrome (as a consequence primarily of abnormal intestinal mucosa) and, as a false-positive study, in patients with large collections of fluid in a third space (i.e., ascites, pleural fluid).
The Schilling test • Is performed by administering 58Co-labeled cobalamin and
collecting urine for 24 h and is dependent on normal renal and bladder function.
• Urinary excretion of cobalamin will reflect cobalamin absorption provided that intrahepatic binding sites for cobalamin are fully occupied.
• To ensure saturation of hepatic cobalamin binding sites so that all absorbed radiolabeled cobalamin will be excreted in urine, 1 mg cobalamin is administered intramuscularly 1 h following ingestion of the radiolabeled cobalamin.
• The Schilling test may be abnormal (usually defined as 10% excretion in 24 h) in pernicious anemia, chronic pancreatitis, blind loop syndrome and ileal disease.
Histologic Findings
Depending on the cause, the histologic features of malabsorption vary.
– A frequently encountered histologic finding is villous atrophy, which is seen in celiac disease, tropical sprue, viral gastroenteritis, bacterial overgrowth, inflammatory bowel disease, immunodeficiency syndromes, lymphoma and radiation enteritis.